群体水平基因型数据与功能注释的整合揭示了长链非编码RNA在卵巢癌易感位点的过度富集。
Integration of Population-Level Genotype Data with Functional Annotation Reveals Over-Representation of Long Noncoding RNAs at Ovarian Cancer Susceptibility Loci.
作者信息
Reid Brett M, Permuth Jennifer B, Chen Y Ann, Teer Jamie K, Monteiro Alvaro N A, Chen Zhihua, Tyrer Jonathan, Berchuck Andrew, Chenevix-Trench Georgia, Doherty Jennifer A, Goode Ellen L, Iverson Edwin S, Lawrenson Kate, Pearce Celeste L, Pharoah Paul D, Phelan Catherine M, Ramus Susan J, Rossing Mary Anne, Schildkraut Joellen M, Cheng Jin Q, Gayther Simon A, Sellers Thomas A
机构信息
Moffitt Cancer Center & Research Institute, Tampa, Florida.
University of Cambridge, Cambridge, United Kingdom.
出版信息
Cancer Epidemiol Biomarkers Prev. 2017 Jan;26(1):116-125. doi: 10.1158/1055-9965.EPI-16-0341. Epub 2016 Dec 29.
BACKGROUND
Genome-wide association studies (GWAS) have identified multiple loci associated with epithelial ovarian cancer (EOC) susceptibility, but further progress requires integration of epidemiology and biology to illuminate true risk loci below genome-wide significance levels (P < 5 × 10). Most risk SNPs lie within non-protein-encoding regions, and we hypothesize that long noncoding RNA (lncRNA) genes are enriched at EOC risk regions and represent biologically relevant functional targets.
METHODS
Using imputed GWAS data from about 18,000 invasive EOC cases and 34,000 controls of European ancestry, the GENCODE (v19) lncRNA database was used to annotate SNPs from 13,442 lncRNAs for permutation-based enrichment analysis. Tumor expression quantitative trait locus (eQTL) analysis was performed for sub-genome-wide regions (1 × 10 > P > 5 × 10) overlapping lncRNAs.
RESULTS
Of 5,294 EOC-associated SNPs (P < 1.0 × 10), 1,464 (28%) mapped within 53 unique lncRNAs and an additional 3,484 (66%) SNPs were correlated (r > 0.2) with SNPs within 115 lncRNAs. EOC-associated SNPs comprised 130 independent regions, of which 72 (55%) overlapped with lncRNAs, representing a significant enrichment (P = 5.0 × 10) that was more pronounced among a subset of 5,401 lncRNAs with active epigenetic regulation in normal ovarian tissue. EOC-associated lncRNAs and their putative promoters and transcription factors were enriched for biologically relevant pathways and eQTL analysis identified five novel putative risk regions with allele-specific effects on lncRNA gene expression.
CONCLUSIONS
lncRNAs are significantly enriched at EOC risk regions, suggesting a mechanistic role for lncRNAs in driving predisposition to EOC.
IMPACT
lncRNAs represent key candidates for integrative epidemiologic and functional studies. Further research on their biologic role in ovarian cancer is indicated. Cancer Epidemiol Biomarkers Prev; 26(1); 116-25. ©2016 AACR.
背景
全基因组关联研究(GWAS)已鉴定出多个与上皮性卵巢癌(EOC)易感性相关的基因座,但进一步的进展需要整合流行病学和生物学,以阐明全基因组显著性水平(P < 5×10)以下的真正风险基因座。大多数风险单核苷酸多态性(SNP)位于非蛋白质编码区域,我们推测长链非编码RNA(lncRNA)基因在EOC风险区域富集,并代表生物学上相关的功能靶点。
方法
利用约18000例侵袭性EOC病例和34000例欧洲血统对照的推测GWAS数据,使用GENCODE(v19)lncRNA数据库对来自13442个lncRNA的SNP进行基于置换的富集分析。对与lncRNA重叠的亚全基因组区域(1×10 > P > 5×10)进行肿瘤表达数量性状基因座(eQTL)分析。
结果
在5294个与EOC相关的SNP(P < 1.0×10)中,1464个(28%)定位于53个独特的lncRNA内,另外3484个(66%)SNP与115个lncRNA内的SNP相关(r > 0.2)。与EOC相关的SNP包含130个独立区域,其中72个(55%)与lncRNA重叠,这代表了显著的富集(P = 5.0×10),在正常卵巢组织中具有活跃表观遗传调控的5401个lncRNA子集中更为明显。与EOC相关的lncRNA及其假定的启动子和转录因子在生物学相关途径中富集,eQTL分析确定了五个新的假定风险区域,这些区域对lncRNA基因表达具有等位基因特异性效应。
结论
lncRNA在EOC风险区域显著富集,表明lncRNA在驱动EOC易感性方面具有机制性作用。
影响
lncRNA代表了综合流行病学和功能研究的关键候选物。表明需要进一步研究它们在卵巢癌中的生物学作用。癌症流行病学、生物标志物与预防;26(1);116 - 25。©2016美国癌症研究协会。
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